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Therapeutic Opportunities with Pharmacological Inhibition of CD38 with Isatuximab

达拉图穆马 CD38 泊马度胺 药理学 抗体 依法利珠单抗 医学 多发性骨髓瘤 单克隆抗体 癌症研究 免疫学 内科学 沙利度胺 生物 干细胞 疾病 细胞生物学 川地34 英夫利昔单抗
作者
Thomas G. Martin,Kathryn P. Corzo,Marielle Chiron,Helgi van de Velde,Giovanni Abbadessa,Frank Campana,Malini Solanki,Robin Meng,Helen Lee,Dmitri Wiederschain,Chen Zhu,Alexey Rak,Kenneth C. Anderson
出处
期刊:Cells [MDPI AG]
卷期号:8 (12): 1522-1522 被引量:145
标识
DOI:10.3390/cells8121522
摘要

CD38 is a transmembrane glycoprotein with ectoenzymatic activity involved in regulation of migration, signal transduction, and receptor-mediated adhesion. CD38 is highly expressed on various malignant cells, including multiple myeloma (MM), and at relatively low levels in other tissues, making it a suitable target for therapeutic antibodies. Several anti-CD38 therapies have been, or are being, developed for the treatment of MM, including daratumumab and isatuximab (SAR650984), respectively. Studies have shown that anti-CD38 therapies are effective in the treatment of relapsed/refractory MM and are well tolerated, with infusion reactions being the most common side effects. They can be used as monotherapy or in combination with immunomodulatory agents, such as pomalidomide, or proteasome inhibitors to potentiate their activity. Here we examine isatuximab and several anti-CD38 agents in development that were generated using new antibody engineering techniques and that may lead to more effective CD38 targeting. We also summarize trials assessing these antibodies in MM, other malignancies, and solid organ transplantation. Finally, we propose that further research on the mechanisms of resistance to anti-CD38 therapy and the development of biomarkers and new backbone regimens with CD38 antibodies will be important steps in building more personalized treatment for patients with MM.
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